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Clinical Genetics

Resumen/Descripción – provisto por la editorial en inglés

Clinical Genetics links research to the clinic, translating advances in our understanding of the molecular basis of genetic disease for the practising clinical geneticist. The journal publishes high quality research papers, short reports, reviews and mini-reviews that connect medical genetics research with clinical practice.

Palabras clave – provistas por la editorial

Clinical Genetics; CGE; genetics; molecular medicine; immunogenetics; medical genetics; gene express

Disponibilidad

Institución detectada	Período	Navegá	Descargá	Solicitá
No detectada	desde ene. 1970 / hasta dic. 2023	Wiley Online Library

Información

Tipo de recurso:

revistas

ISSN impreso

0009-9163

ISSN electrónico

1399-0004

Editor responsable

John Wiley & Sons, Inc. (WILEY)

País de edición

Estados Unidos

Fecha de publicación

1970-

Cobertura temática

Medicina básica

Biotecnología médica

Tabla de contenidos

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doi: 10.1111/cge.14148

Carrier frequency of autosomal recessive genetic conditions in diverse populations: Lessons learned from the genome aggregation database

Matthew J. Schmitz; Mahmoud Aarabi; Ali Bashar; Aleksandar Rajkovic; Anthony R. Gregg; Svetlana A. Yatsenko

Palabras clave: Genetics (clinical); Genetics.

Pp. 87-97

doi: 10.1111/cge.14249

New Cerebellar Ataxia, Neuropathy, Vestibular Areflexia Syndrome cases are caused by the presence of a nonsense variant in compound heterozygosity with the pathogenic repeat expansion in the RFC1

Ana Arteche‐López; Almudena Avila‐Fernandez; Alejandra Damian; Emma Soengas‐Gonda; Rubén Pérez de la Fuente; Patricia Ramos Gómez; Jesús Gallego Merlo; Laura Horcajada Burgos; Carlos Cemillán Fernández; Jose Miguel Lezana Rosales; Juan Francisco González Martínez; Juan Francisco Quesada‐Espinosa; Marta Corton; Maria Paz Guerrero‐Molina

Palabras clave: Genetics (clinical); Genetics.

Pp. 236-241

doi: 10.1111/cge.14423

Lamb–Shaffer syndrome: 20 Spanish patients and literature review expands the view of neurodevelopmental disorders caused by SOX5 haploinsufficiency

Jair Tenorio‐Castano; Ángela Sánchez‐Algaba Gómez; Mónica Coronado; Pilar Rodríguez‐Martín; Alejandro Parra; Patricia Pascual; Mario Cazalla; Natalia Gallego; Pedro Arias; Aixa V. Morales; Julián Nevado; Pablo Lapunzina

<jats:title>Abstract</jats:title><jats:p>Lamb–Shaffer Syndrome (LSS; OMIM #616803; ORPHA #313892; ORPHA #313884) is an infrequent genetic disorder that affects multiple aspects of human development especially those related to the development of the nervous system. LSS is caused by variants in the <jats:italic>SOX5</jats:italic> gene. At the molecular level, <jats:italic>SOX5</jats:italic> gene encodes for a transcription factor containing a High Mobility Group (HMG) DNA‐Binding domain with relevant functions in brain development in different vertebrate species. Clinical features of Lamb–Shaffer syndrome may include intellectual disability, delayed speech and language development, attention deficits, hyperactivity, autism spectrum disorder, visual problems and seizures. Additionally, patients with the syndrome may present distinct facial dimorphism such as a wide mouth with full lips, small chin, broad nasal bridge, and deep‐set eyes. Other physical features that have been reported in some patients include short stature, scoliosis, and joint hypermobility. Here, we report the clinical and molecular characterization of a Spanish LSS cohort of new 20 patients and review all the patients published so far which amount for 111 patients. The most frequent features included developmental delay, intellectual disability, visual problems, poor speech development and facial dysmorphic features. Strikingly, pain insensitivity and hypermetropia seems to be more frequent than previously reported, based on the frequency seen in the Spanish cohort. Eighty‐three variants have been reported so far, single nucleotide variants (SNV) and copy number variants represent 47% and 53%, respectively, from the total of variants reported. Similarly to previous reports, the majority of the SNVs variants of the novel patients reported herein fall in the HMG domain of the protein. However, new variants, affecting other functional domains, were also detected. In conclusion, LLS is a rare genetic disorder mostly characterized by a wide range of developmental and neurological symptoms. Early diagnosis would allow to start of care programs, clinical follow up, prospective studies and appropriate genetic counseling, to promote clinical and social improvement to have profound lifelong benefits for patients and their families. Further research is needed to better understand the underlying mechanisms of the syndrome related to <jats:italic>SOX5</jats:italic> haploinsufficiency.</jats:p>

Palabras clave: Genetics (clinical); Genetics.

Pp. 637-647